Literature DB >> 17638875

Cancer cells and normal cells differ in their requirements for Thoc1.

Yanping Li1, Athena W Lin, Xiaojing Zhang, Yanqing Wang, Xiaoling Wang, David W Goodrich.   

Abstract

The evolutionarily conserved TREX (Transcription/Export) complex physically couples transcription, messenger ribonucleoprotein particle biogenesis, RNA processing, and RNA export for a subset of genes. HPR1 encodes an essential component of the S. cerevisiae TREX complex. HPR1 loss compromises transcriptional elongation, nuclear RNA export, and genome stability. Yet, HPR1 is not required for yeast viability. Thoc1 is the recently discovered human functional orthologue of HPR1. Thoc1 is expressed at higher levels in breast cancer than in normal epithelia, and expression levels correlate with tumor size and metastatic potential. Depletion of Thoc1 protein (pThoc1) in human cancer cell lines compromises cell proliferation. It is currently unclear whether Thoc1 is essential for all mammalian cells or whether cancer cells may differ from normal cells in their dependence on Thoc1. To address this issue, we have compared the requirements for Thoc1 in the proliferation and survival of isogenic normal and oncogene-transformed cells. Neoplastic cells rapidly lose viability via apoptotic cell death on depletion of pThoc1. Induction of apoptotic cell death is coincident with increased DNA damage as indicated by the appearance of phosphorylated histone H2AX. In contrast, the viability of normal cells is largely unaffected by pThoc1 loss. Normal cells lacking Thoc1 cannot be transformed by forced expression of E1A and Ha-ras, suggesting that Thoc1 may be important for neoplastic transformation. In sum, our data are consistent with the hypothesis that cancer cells require higher levels of pThoc1 for survival than normal cells. If true, pThoc1 may provide a novel molecular target for cancer therapy.

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Year:  2007        PMID: 17638875      PMCID: PMC2804983          DOI: 10.1158/0008-5472.CAN-06-3234

Source DB:  PubMed          Journal:  Cancer Res        ISSN: 0008-5472            Impact factor:   12.701


  35 in total

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Authors:  Yanping Li; Xiaoling Wang; Xiaojing Zhang; David W Goodrich
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  25 in total

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5.  Background gene expression networks significantly enhance drug response prediction by transcriptional profiling.

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6.  The Thoc1 ribonucleoprotein and prostate cancer progression.

Authors:  Meenalakshmi Chinnam; Yanqing Wang; Xiaojing Zhang; David L Gold; Thaer Khoury; Alexander Yu Nikitin; Barbara A Foster; Yanping Li; Wiam Bshara; Carl D Morrison; Rochelle D Payne Ondracek; James L Mohler; David W Goodrich
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Review 7.  The RB/E2F pathway and regulation of RNA processing.

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Authors:  Annalisa Mancini; Susanne C Niemann-Seyde; Rüdiger Pankow; Omar El Bounkari; Sabine Klebba-Färber; Alexandra Koch; Ewa Jaworska; Elaine Spooncer; Achim D Gruber; Anthony D Whetton; Teruko Tamura
Journal:  BMC Biol       Date:  2010-01-05       Impact factor: 7.431

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